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首页> 外文期刊>American Journal of Transplantation >Decay Accelerating Factor is Essential for Successful Corneal Engraftment
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Decay Accelerating Factor is Essential for Successful Corneal Engraftment

机译:衰变加速因子对于成功植入角膜至关重要

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摘要

In contrast to immune restrictions that pertain for solid organ transplants, the tolerogenic milieu of the eye permits successful corneal transplantation without systemic immunosuppression, even across a fully MHC disparate barrier. Here we show that recipient and donor expression of decay accelerating factor (DAF or CD55), a cell surface C3/C5 convertase regulator recently shown to modulate T-cell responses, is essential to sustain successful corneal engraftment. Whereas wild-type (WT) corneas transplanted into multiple minor histocompatibility antigen (mH), or HY disparate WT recipients were accepted, DAF's absence on either the donor cornea or in the recipient bed induced rapid rejection. Donor or recipient DAF deficiency led to expansion of donor-reactive IFN- producing CD4+ and CD8+ T cells, as well as inhibited antigen-induced IL-10 and TGF-β, together demonstrating that DAF deficiency precludes immune tolerance. In addition to demonstrating a requisite role for DAF in conferring ocular immune privilege, these results raise the possibility that augmenting DAF levels on donor corneal endothelium and/or the recipient bed could have therapeutic value for transplants that clinically are at high risk for rejection.
机译:与实体器官移植相关的免疫限制相反,眼睛的致耐受性环境允许成功进行角膜移植,而无需全身免疫抑制,即使跨越完全MHC完全不同的屏障也是如此。在这里,我们显示了衰变加速因子(DAF或CD55)的受体和供体表达,它是最近被证明可调节T细胞反应的细胞表面C3 / C5转化酶调节剂,对于维持成功的角膜植入至关重要。接受移植到多个次要组织相容性抗原(mH)或HY不同的WT受体中的野生型(WT)角膜,而在供体角膜或受体床上缺乏DAF会导致快速排斥。供体或受体DAF缺乏导致供体反应性产生IFN的CD4 + 和CD8 + T细胞扩增,并抑制了抗原诱导的IL-10和TGF- β一起证明DAF缺乏会阻止免疫耐受。除了证明DAF在赋予眼部免疫特权方面所起的必要作用外,这些结果还增加了增加供体角膜内皮和/或受体床上DAF水平对临床上具有高排斥反应风险的移植物具有治疗价值的可能性。

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